Targeting Mitochondrial Impairment in Parkinson's Disease: Challenges and Opportunities

Prasuhn, Jannik; Davis, Ryan L.; Kumar, Kishore R.

doi:10.3389/fcell.2020.615461

Cited by 96 publications

(77 citation statements)

References 199 publications

(201 reference statements)

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“…In contrast, as a generic term, "mitochondrial dysfunction" oversimplifies the multifaceted nature of mitochondrial biology in health and disease. PD-associated mitochondrial dysfunction presents with a variety of molecular events, including impaired mitochondrial biogenesis, increased release of reactive oxygen species (ROS), defective mitophagy and trafficking, electron transport chains (ETC) dysfunction, variations in mitochondrial dynamics, calcium (Ca2+) imbalance, neuroinflammation, and possible indirect influences on mitochondrial homeostasis from presumably unrelated pathways (e.g., alpha-synuclein deposition) [8]. The centrality of mitochondria in cellular functioning and the convergence of mammalian metabolism on mitochondria suggest that potential therapies must address a complex web of interconnected pathways [9].…”

Section: Mitochondrial Dysfunction In Idiopathic and Monogenic Parkinson's Diseasementioning

confidence: 99%

“…A promising approach can derive from enhanced insights into the individual disease genetics (e.g., by presymptomatic genetic testing or polygenetic risk scoring) [133]. However, blood-or neuroimaging-based assessments of mitochondrial dysfunction can substantially enhance our current understanding of mitochondrial dysfunction's temporal and spatial dynamics in vivo [8]. Current knowledge gaps of essential aspects of mitochondrial biology need to be closed for the rational design of gene therapies.…”

Section: Special Considerations For Mitochondrial Gene Therapymentioning

confidence: 99%

“…PD: Parkinson's disease. The table has been adapted and modified from Prasuhn et al[8].2.1.2. Gene repair and enhancement of nuclear-encoded mitochondrial genes.…”

mentioning

confidence: 99%

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Gene Therapeutic Approaches for the Treatment of Mitochondrial Dysfunction in Parkinson’s Disease

Prasuhn

Brüggemann

2021

Preprint

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Background. Mitochondrial dysfunction has been identified as a pathophysiological hallmark of disease onset and progression in patients with Parkinsonian disorders. Besides the overall emergence of gene therapies in treating these patients, this highly relevant molecular concept has not yet been defined as a target for gene therapeutic approaches. Methods. This narrative review will discuss the experimental evidence suggesting mitochondrial dysfunction as a viable treatment target in patients with monogenic and idiopathic Parkinson’s disease. In addition, we will focus on general treatment strategies and crucial challenges which need to be overcome. Results. Our current understanding of mitochondrial biology in parkinsonian disorders opens up the avenue for viable treatment strategies in Parkinsonian disorders. Insights can be obtained from primary mitochondrial diseases. However, substantial knowledge gaps and unique challenges of mitochondria-targeted gene therapies need to be addressed to provide innovative treatments in the future. Conclusions. Mitochondria-targeted gene therapies are a potential strategy to improve an important primary disease mechanism in Parkinsonian disorders. However, further studies are needed to address the unique design challenges for mitochondria-targeted gene therapies.

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Section: Mitochondrial Dysfunction In Idiopathic and Monogenic Parkinson's Diseasementioning

confidence: 99%

Section: Special Considerations For Mitochondrial Gene Therapymentioning

confidence: 99%

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Gene Therapeutic Approaches for the Treatment of Mitochondrial Dysfunction in Parkinson’s Disease

Prasuhn

Brüggemann

2021

Preprint

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“…PARK2 and PARK6, which encode for parkin and PINK1 respectively, are genes responsible of the onset of familial Parkinson's disease (PD) a progressive degenerative disorder of the central nervous system characterized by dopaminergic neurodegeneration in the substantia nigra pars compacta. Several studies in PD models proved hallmarked dysfunctions of mitochondria, in particular, defect of the respiratory chain complex I, which plays a central role in mitochondrial oxidative phosphorylation (OXPHOS) efficiency and capacity [1], depletion of ATP production, increased reactive oxygen species (ROS) and oxidative stress, anomalies in mitochondrial dynamics, trafficking and turnover, dysregulation in calcium homeostasis, and protein misfolding and aggregation [2][3][4][5][6][7][8][9][10].…”

Section: Introductionmentioning

confidence: 99%

Resveratrol Treatment in Human Parkin-Mutant Fibroblasts Modulates cAMP and Calcium Homeostasis Regulating the Expression of Mitochondria-Associated Membranes Resident Proteins

et al. 2021

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Parkin plays an important role in ensuring efficient mitochondrial function and calcium homeostasis. Parkin-mutant human fibroblasts, with defective oxidative phosphorylation activity, showed high basal cAMP level likely ascribed to increased activity/expression of soluble adenylyl cyclase and/or low expression/activity of the phosphodiesterase isoform 4 and to a higher Ca2+ level. Overall, these findings support the existence, in parkin-mutant fibroblasts, of an abnormal Ca2+ and cAMP homeostasis in mitochondria. In our previous studies resveratrol treatment of parkin-mutant fibroblasts induced a partial rescue of mitochondrial functions associated with stimulation of the AMPK/SIRT1/PGC-1α pathway. In this study we provide additional evidence of the potential beneficial effects of resveratrol inducing an increase in the pre-existing high Ca2+ level and remodulation of the cAMP homeostasis in parkin-mutant fibroblasts. Consistently, we report in these fibroblasts higher expression of proteins implicated in the tethering of ER and mitochondrial contact sites along with their renormalization after resveratrol treatment. On this basis we hypothesize that resveratrol-mediated enhancement of the Ca2+ level, fine-tuned by the ER–mitochondria Ca2+ crosstalk, might modulate the pAMPK/AMPK pathway in parkin-mutant fibroblasts.

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“…Also, studies performed in postmortem PD patient brain tissue have shown decreased mitochondrial biomass, bioenergetic capacity, and altered mitochondrial distribution of mitochondria within the cell bodies and neurites ( Schapira et al, 1990 ; Keeney et al, 2006 ; Navarro et al, 2009 ; Mallach et al, 2019 ). Thus, therapies that reverse mitochondrial dysfunction are a promising therapeutic approach; however, various human clinical trials targeting mitochondrial dysfunction in PD have been unsuccessful in reversing the course of disease (e.g., disease progression and motor symptoms) ( Beal et al, 2014 ; Kieburtz et al, 2015 ; Prasuhn et al, 2021 ). Thereby, additional basic science studies that functionally dissect the role of the various mitochondrial localized PD-linked gene products and their function are essential to broaden our understanding of mitochondria and their role in PD pathogenesis, ultimately leading to targeted therapies against PD.…”

Section: Introductionmentioning

confidence: 99%

Role of Cleaved PINK1 in Neuronal Development, Synaptogenesis, and Plasticity: Implications for Parkinson’s Disease

Soman

Dagda

2021

Front. Neurosci.

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Mitochondrial dysfunction plays a significant role in the pathogenesis of Parkinson’s disease (PD). Consistent with this concept, loss of function mutations in the serine/threonine kinase- PINK1 (PTEN-induced putative kinase-1) causes autosomal recessive early onset PD. While the functional role of f-PINK1 (full-length PINK1) in clearing dysfunctional mitochondria via mitophagy is extensively documented, our understanding of specific physiological roles that the non-mitochondrial pool of PINK1 imparts in neurons is more limited. PINK1 is proteolytically processed in the intermembrane space and matrix of the mitochondria into functional cleaved products (c-PINK1) that are exported to the cytosol. While it is clear that posttranslational processing of PINK1 depends on the mitochondria’s oxidative state and structural integrity, the functional roles of c-PINK1 in modulating neuronal functions are poorly understood. Here, we review the diverse roles played by c-PINK1 in modulating various neuronal functions. Specifically, we describe the non-canonical functional roles of PINK1, including but not limited to: governing mitochondrial movement, neuronal development, neuronal survival, and neurogenesis. We have published that c-PINK1 stimulates neuronal plasticity and differentiation via the PINK1-PKA-BDNF signaling cascade. In addition, we provide insight into how mitochondrial membrane potential-dependent processing of PINK1 confers conditional retrograde signaling functions to PINK1. Further studies delineating the role of c-PINK1 in neurons would increase our understanding regarding the role played by PINK1 in PD pathogenesis.

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Targeting Mitochondrial Impairment in Parkinson's Disease: Challenges and Opportunities

Cited by 96 publications

References 199 publications

Gene Therapeutic Approaches for the Treatment of Mitochondrial Dysfunction in Parkinson’s Disease

Gene Therapeutic Approaches for the Treatment of Mitochondrial Dysfunction in Parkinson’s Disease

Resveratrol Treatment in Human Parkin-Mutant Fibroblasts Modulates cAMP and Calcium Homeostasis Regulating the Expression of Mitochondria-Associated Membranes Resident Proteins

Role of Cleaved PINK1 in Neuronal Development, Synaptogenesis, and Plasticity: Implications for Parkinson’s Disease

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